Researchers closer to early lung cancer detection

Sam Hanash leads discovery of blood proteins associated with early development of lung cancer; findings hold promise of a blood test for screening, diagnosis

Sept. 19, 2011

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By Kristen Woodward

Dr. Samir Hanash, head of the Molecular Diagnostics Program in the Public Health Sciences Division, led the study.

Center News file photo

A Hutchinson Center team has discovered proteins in the blood that are associated with early lung cancer development in mice and humans. The advance brings the reality of a blood test for the early detection and diagnosis of lung cancer a step closer.

The findings, by a team led by Dr. Samir Hanash, head of the Molecular Diagnostics Program in the Public Health Sciences Division, appear in the Sept. 13 edition of Cancer Cell.

"A major feature of this study was that we were able to replicate findings from mouse models of lung cancer in blood samples from humans with lung cancer both at the time of diagnosis and, importantly, prior to the onset of symptoms and diagnosis," Hanash said. "Our data showed that the protein markers that were tested showed similar concordance between lung cancer in the mouse and lung cancer in humans. This means that developing a blood test to detect lung cancer is increasingly within reach."

The blood protein signatures discovered may be used in the future in a blood test to screen for lung cancer among high-risk individuals such as current and former smokers, and to aid in diagnosis, distinguishing between various subtypes of the disease, such as small-cell lung cancer and lung adenocarcinoma.

Hanash envisions that such a test could be used together with imaging technologies such as CT screening to monitor people at high risk of developing the disease. "There is a substantial need for simple, noninvasive means to detect lung cancer. While imaging-based screening to detect lung cancer has shown promise, blood-based diagnostics provide a complementary means for detection, disease classification, and monitoring for cancer progression and regression," the authors wrote.

Protein signatures specific to lung cancer

For the study, the researchers conducted in-depth blood protein analysis of three mouse models of lung adenocarcinoma and a genetically engineered mouse model of small-cell lung cancer. To further refine the results, they compared these lung cancer protein profiles to those from other well-established mouse models of pancreatic, ovarian, colon, prostate and breast cancer, as well as two mouse models of inflammation without the presence of cancer. Several protein signatures emerged that were specific to lung cancer:

In models of lung adenocarcinoma, the researchers uncovered a set of elevated proteins that are regulated by the NKX2.1 transcription factor, which has been linked to lung development and function. They also discovered a network of dysregulated proteins linked to epidermal growth factor receptor which, when mutated in lung tissue, is associated with cancer development. Levels of these proteins returned to near normal upon treatment with a tyrosine kinase inhibitor, an anti-cancer drug.

In a model of small-cell lung cancer, the researchers found a distinct blood protein signature that was associated with neuroendocrine development.

Analysis shows strong parallels to human cancer

To determine whether these protein signatures in mice were relevant to human lung cancer, the researchers analyzed blood samples from 28 smokers who had been newly diagnosed with operable lung cancer and blood samples from 26 other subjects that were obtained up to a year before lung cancer was diagnosed. For comparison purposes they also analyzed blood from a similar number of matched, cancer-free controls.

The researchers found striking similarities between the protein signatures in mice and human. For example, in mice with small-cell lung cancer, they found elevated levels of a neural protein called Robo1. They also found significantly increased levels of this protein in patients with small-cell lung cancer as compared to matched human controls.

"Additional validation studies are in progress to further determine the sensitivity and specificity of the marker panels," Hanash said.

In addition to co-author Dr. Harold Varmus, director of the National Cancer Institute, collaborators included researchers from Memorial Sloan-Kettering Cancer Center, the National Human Genome Research Institute, Yale University School of Medicine, Stanford University, the University of Texas Southwestern Medical Center, and Brigham and Women’s Hospital and Dana-Farber Cancer Institute, Harvard Medical School.

Funding for the research came from the NCI Mouse Models of Human Cancer Program, the NCI Early Detection Research Network, the Canary Foundation, the Thomas G. Labrecque Foundation, the Uniting Against Lung Cancer Foundation, the Department of Defense Congressionally Directed Lung Cancer Research Program and the Parker B. Francis Fellowship Program of the Francis Family Foundation.